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High-frequency intracellular infection and erythrogenic toxin A expression undergo phase variation in M1 group A streptococci.

机译:在M1组A链球菌中,高频细胞内感染和血红蛋白毒素A表达发生相变。

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摘要

A clonal variant of serotype M1 group A streptococcus, strain 90-131, disseminated to several continents, where it was associated with severe systemic infections and toxic shock. Although this strain harbours the speA gene and is efficiently internalized by human epithelial cells, clinical isolates often fail to express the erythrogenic toxin under laboratory growth conditions. Cultures of strain 90-131 were observed to phase vary between small, dry, compact and larger, more mucoid colonies. The former were shown to be poorly internalized by epithelial cells. Analysis of RNA by Northern hybridization demonstrated that the emml, hasA and speA genes were weakly transcribed in cultures derived from the small colonies and highly transcribed in those derived from the large colonies. An insertion mutation in mga (the multigene activator) downregulated the invasion of epithelial cells and the transcription of emm1 and hasA, but had little impact on the transcription of speA. These are the first data to suggest the existence of a common regulatory circuit linking intracellular invasion, M protein, hyaluronic acid capsule and erythrogenic toxin expression by group A streptococcus. Moreover, the genetic instability of toxin expression exhibited by this serotype may impact on laboratory studies that attempt to associate toxin production with toxic shock.
机译:血清型M1 A组链球菌的克隆变体,菌株90-131,已传播到多个大陆,与严重的全身感染和中毒性休克有关。尽管该菌株带有speA基因并被人上皮细胞有效地内在化,但临床分离株在实验室生长条件下常常无法表达促红细胞生成素。观察到菌株90-131的培养物在小的,干燥的,紧密的和更大的,更多的粘液样菌落之间发生相变。前者被上皮细胞内化性差。通过Northern杂交对RNA的分析表明,emml,hasA和speA基因在小菌落衍生的培养物中被弱转录,而在大菌落衍生的培养物中被高转录。 mga(多基因激活剂)中的插入突变下调了上皮细胞的侵袭以及emm1和hasA的转录,但对speA的转录影响很小。这些是第一个数据,表明存在一个共同的调节回路,该回路将细胞内侵袭,M蛋白,透明质酸胶囊和A组链球菌的红血球毒素表达联系起来。而且,这种血清型表现出的毒素表达的遗传不稳定性可能会影响将毒素产生与中毒性休克联系起来的实验室研究。

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